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基于结构的水力压裂化学品作为新型雄激素受体拮抗剂的内分泌干扰作用的发现。

Structure-based discovery of the endocrine disrupting effects of hydraulic fracturing chemicals as novel androgen receptor antagonists.

机构信息

Department of Environmental Toxicology, University of California, Davis, CA, 95616, USA.

Molecular Graphics and Computation Facility, College of Chemistry, University of California, Berkeley, CA, 94720, USA.

出版信息

Chemosphere. 2020 Oct;257:127178. doi: 10.1016/j.chemosphere.2020.127178. Epub 2020 May 27.

Abstract

Hydraulic fracturing (HF) technology is increasingly utilized for oil and gas extraction operations. The widespread use of HF has led to concerns of negative impacts on both the environment and human health. Indeed, the potential endocrine disrupting impacts of HF chemicals is one such knowledge gap. Herein, we used structure-based molecular docking to assess the binding affinities of 60 HF chemicals to the human androgen receptor (AR). Five HF chemicals had relatively high predicted AR binding affinity, suggesting the potential for endocrine disruption. We next assessed androgenic and antiandrogenic activities of these chemicals in vitro. Of the five candidate AR ligands, only Genapol®X-100 significantly modified AR transactivation. To better understand the structural effect of Genapol®X-100 on the potency of AR inhibition, we compared the antiandrogenic activity of Genapol®X-100 with that of its structurally similar chemical, Genapol®X-080. Interestingly, both Genapol®X-100 and Genapol®X-080 elicited an antagonistic effect at AR with 20% relative inhibitory concentrations of 0.43 and 0.89 μM, respectively. Furthermore, we investigated the mechanism of AR inhibition of these two chemicals in vitro, and found that both Genapol®X-100 and Genapol®X-080 inhibited AR through a noncompetitive mechanism. The effect of these two chemicals on the expression of AR responsive genes, e.g. PSA, KLK2, and AR, was also investigated. Genapol®X-100 and Genapol®X-080 altered the expression of these genes. Our findings heighten awareness of endocrine disruption by HF chemicals and provide evidence that noncompetitive antiandrogenic Genapol®X-100 could cause adverse endocrine health effects.

摘要

水力压裂(HF)技术越来越多地用于石油和天然气开采作业。HF 的广泛使用引起了人们对环境和人类健康的负面影响的关注。事实上,HF 化学物质潜在的内分泌干扰影响就是这样一个知识空白。在这里,我们使用基于结构的分子对接来评估 60 种 HF 化学物质与人雄激素受体(AR)的结合亲和力。五种 HF 化学物质具有相对较高的预测 AR 结合亲和力,表明它们具有潜在的内分泌干扰能力。我们接下来评估了这些化学物质在体外的雄激素和抗雄激素活性。在这五种候选 AR 配体中,只有 Genapol®X-100 显著改变了 AR 的转录激活。为了更好地理解 Genapol®X-100 对 AR 抑制效力的结构影响,我们比较了 Genapol®X-100 和其结构相似的化学物质 Genapol®X-080 的抗雄激素活性。有趣的是,Genapol®X-100 和 Genapol®X-080 都对 AR 产生了拮抗作用,其 20%相对抑制浓度分别为 0.43 和 0.89μM。此外,我们研究了这两种化学物质在体外对 AR 抑制的作用机制,发现 Genapol®X-100 和 Genapol®X-080 都通过非竞争性机制抑制 AR。我们还研究了这两种化学物质对 AR 响应基因,如 PSA、KLK2 和 AR 的表达的影响。Genapol®X-100 和 Genapol®X-080 改变了这些基因的表达。我们的发现提高了对 HF 化学物质引起内分泌干扰的认识,并提供了证据表明非竞争性抗雄激素 Genapol®X-100 可能会对内分泌健康产生不利影响。

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